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控制人类脂肪组织发育的分子机制:从单基因突变性脂肪营养不良症中获得的启示。

Molecular mechanisms controlling human adipose tissue development: insights from monogenic lipodystrophies.

机构信息

Metabolic Research Laboratories, Institute of Metabolic Science, University of Cambridge, Addenbrookes Hospital, Hills Road Cambridge, Cambridge CB2 0QQ, UK.

出版信息

Expert Rev Mol Med. 2010 Aug 2;12:e24. doi: 10.1017/S1462399410001547.

Abstract

Appropriately functioning adipose tissue is essential for human health, a fact most clearly illustrated by individuals with lipodystrophy, who have impaired adipose development and often suffer severe metabolic disease as a result. Humans with obesity display a similar array of metabolic problems. This reflects failures in fat tissue function in obesity, which results in consequences similar to those seen when insufficient adipose tissue is present. Thus a better understanding of the molecules that regulate the development of fat tissue is likely to aid the generation of novel therapeutic strategies for the treatment of all disorders of altered fat mass. Single gene disruptions causing lipodystrophy can give unique insights into the importance of the proteins they encode in human adipose tissue development. Moreover, the mechanisms via which they cause lipodystrophy can reveal new molecules and pathways important for adipose tissue development and function as well as confirming the importance of molecules identified from studies of cellular and animal models.

摘要

适当功能的脂肪组织对人类健康至关重要,这一事实在脂肪营养不良患者身上表现得最为明显,他们的脂肪发育受损,常常因此患上严重的代谢疾病。肥胖症患者表现出类似的一系列代谢问题。这反映了肥胖症中脂肪组织功能的失败,其结果与脂肪组织不足时所产生的后果相似。因此,更好地了解调节脂肪组织发育的分子可能有助于为治疗所有改变脂肪量的疾病生成新的治疗策略。导致脂肪营养不良的单一基因突变可以深入了解它们在人类脂肪组织发育中所编码的蛋白质的重要性。此外,它们导致脂肪营养不良的机制可以揭示新的分子和途径,这些对脂肪组织的发育和功能很重要,同时也证实了从细胞和动物模型研究中确定的分子的重要性。

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